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周细胞包被雷帕霉素微球促进长期猪静脉动脉间置移植后静脉病变。

Periadventitial rapamycin-eluting microbeads promote vein graft disease in long-term pig vein-into-artery interposition grafts.

机构信息

Bristol Heart Institute, University of Bristol, Bristol, United Kingdom.

出版信息

Circ Cardiovasc Interv. 2010 Apr;3(2):157-65. doi: 10.1161/CIRCINTERVENTIONS.109.864660. Epub 2010 Mar 23.

Abstract

BACKGROUND

Neointima formation and atherosclerosis compromise long-term graft patency in aortocoronary and peripheral vein bypass grafts. We investigated the short- and long-term effects of periadventitial application of a sustained-release formulation of rapamycin on experimental pig vein grafts with similar dimensions and kinetics to human saphenous vein bypass grafts.

METHODS AND RESULTS

Periadventitial application of rapamycin-eluting polyvinyl alcohol microspheres (60 microg . cm(-2)) to porcine saphenous vein-to-carotid artery interposition grafts inhibited vein graft positive and vascular smooth muscle cell proliferation in 1-week grafts. It also decreased neointima formation and wall thickening in 4-week vein grafts compared with controls. The inhibition of vein graft thickening was not sustained; however, a catch-up phenomenon was observed, and there was no therapeutic benefit evident in 12-week grafts. Increasing the dose of rapamycin to 120 microg . cm(-2) was associated with significant local toxicity manifest by high rates of graft rupture (25%), inhibition of adventitial neoangiogenesis, and a paradoxical acceleration of vein graft disease as evidenced by increased vascular smooth muscle cell proliferation.

CONCLUSIONS

Local toxicity and poor long-term efficacy limits the clinical applicability of locally applied, sustained rapamycin release in vein graft disease.

摘要

背景

新内膜形成和动脉粥样硬化会损害冠状动脉和外周静脉旁路移植的长期通畅性。我们研究了包绕在血管周围给予雷帕霉素持续释放制剂对实验猪静脉移植物的短期和长期影响,这些移植物在尺寸和动力学方面与人类大隐静脉旁路移植物相似。

方法和结果

将雷帕霉素洗脱聚乙烯醇微球(60 微克/cm2)包绕在猪大隐静脉至颈动脉间置移植术中,可抑制 1 周时移植静脉的正性重塑和血管平滑肌细胞增殖。与对照组相比,它还可减少 4 周时的新生内膜形成和血管壁增厚。然而,对静脉移植物增厚的抑制并不持久,出现追赶现象,12 周时没有明显的治疗效果。增加雷帕霉素的剂量至 120 微克/cm2 会导致局部毒性显著增加,表现为较高的移植物破裂率(25%)、抑制外膜新生血管形成以及静脉移植物疾病的反常加速,表现为血管平滑肌细胞增殖增加。

结论

局部毒性和较差的长期疗效限制了局部应用雷帕霉素持续释放治疗静脉移植物疾病的临床适用性。

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